Department of Ophthalmology, Mayo Clinic, Rochester, Minnesota.
Department of Neurology, Mayo Clinic, Rochester, Minnesota.
JAMA Ophthalmol. 2021 Jun 1;139(6):658-662. doi: 10.1001/jamaophthalmol.2021.0651.
The clinical utility of most antiretinal antibodies (retina antibodies) currently available for testing remains unclear and unproven. Despite this, the presence of retinal antibodies is included in current diagnostic autoimmune retinopathy criteria.
To evaluate the clinical significance of comprehensive retinal antibody evaluations currently offered in North America.
DESIGN, SETTING, AND PARTICIPANTS: In this cross-sectional study, 14 patients without autoimmune retinopathy were recruited into the Mayo Clinic Neuroimmunology Biorepository for this study between January 1, 2019, and October 1, 2019. These serum samples without autoimmune retinopathy were sent in masked fashion to a Clinical Laboratory Improvement Amendments-certified laboratory. Using similar methods, the Mayo Clinic Neuroimmunology Research Laboratory independently assessed the same sample to ascertain reproducibility of the findings.
Results of the autoimmune retinopathy and cancer-associated retinopathy panels.
Thirteen of 14 (93%; 95% CI, 66%-100%) serum samples tested positive for retinal antibodies, with a median of 5 retinal antibodies (range, 0-8) per patient at the Clinical Laboratory Improvement Amendments-certified laboratory, which provides a specificity of 7% (95% CI, 0%-34%). Confirmatory immunohistochemistry staining in human retina was present in 12 of 14 samples (86%). α-Enolase was found in 9 (64%). The only retinal antibody not present was recoverin. These nonspecific retinal antibody results were replicated at the Mayo Clinic Laboratory on Western blot using pig retina proteins as substrate.
The presence of retinal antibodies in 93% of the patients without autoimmune retinopathy indicates a lack of specificity and that most detectable retinal antibodies have limited clinical relevance in the evaluation of patients for suspected autoimmune retinopathy. Current retinal antibody testing, other than recoverin, should be interpreted with caution, especially for cases of low clinical suspicion. The poor specificity is important to recognize to prevent the potentially unnecessary commencement of systemic immunosuppressants that may result in significant extraocular adverse effects. Identification of biomarkers that have a high predictive value for inflammatory or autoimmune retinal diseases is needed to move the field forward.
目前可用于检测的大多数抗视网膜抗体(视网膜抗体)的临床实用性仍不清楚且未经证实。尽管如此,视网膜抗体的存在仍包含在当前的自身免疫性视网膜炎诊断标准中。
评估目前在北美提供的全面视网膜抗体评估的临床意义。
设计、设置和参与者:在这项横断面研究中,2019 年 1 月 1 日至 2019 年 10 月 1 日期间,14 名无自身免疫性视网膜炎的患者被招募到梅奥诊所神经免疫学生物库进行这项研究。这些无自身免疫性视网膜炎的血清样本以盲法送至经临床实验室改进修正案认证的实验室。使用类似的方法,梅奥诊所神经免疫学研究实验室独立评估了相同的样本,以确定发现的可重复性。
自身免疫性视网膜炎和癌症相关视网膜炎检测面板的结果。
在经临床实验室改进修正案认证的实验室中,14 份血清样本中的 13 份(93%;95%CI,66%-100%)检测出视网膜抗体阳性,每位患者的中位数为 5 种视网膜抗体(范围 0-8),特异性为 7%(95%CI,0%-34%)。在 14 个样本中的 12 个(86%)中发现了确认的免疫组织化学染色。α-烯醇酶存在于 9 个样本中(64%)。唯一不存在的视网膜抗体是回收蛋白。这些非特异性视网膜抗体结果在梅奥诊所实验室使用猪视网膜蛋白作为底物的 Western blot 上得到了复制。
在没有自身免疫性视网膜炎的患者中,93%的患者存在视网膜抗体表明缺乏特异性,并且在评估疑似自身免疫性视网膜炎患者时,大多数可检测到的视网膜抗体的临床相关性有限。除回收蛋白外,目前的视网膜抗体检测应谨慎解读,尤其是在临床怀疑程度较低的情况下。特异性差很重要,可防止不必要地开始使用可能导致显著眼外不良反应的全身性免疫抑制剂。需要识别具有高预测价值的生物标志物,以推动该领域的发展。